Targeted gene(s)/phenotype under study
RBM10 (OMIM 300080)
Abstract
Loss of function variants in RBM10 are well known to cause TARP-syndrome, a severe X-linked recessive syndrome with malformations, global developmental delay, and early death of affected males. Missense variants in the RBM10-gene have so far not been proven to be pathogenic. We have collected a cohort of families with RBM10-variants – missense variants, splice variants and loss of function variants – and we are conducting a PhD study of the genotype-phenotype correlation and supporting functional studies.
We welcome further cases of rare variants in the RBM10-gene – all types of variants are included.
Coordinating clinician/researcher
Christina Fagerberg
Institution
Department of Clinical Genetics
Odense University Hospital
Odense, Denmark
Specific requirements beyond clinical data and genotype data sharing
- Re-analysis of DNA samples : No
- Resampling of patients : Yes
- Linked to a translational/basic research project? Yes